Advanced Healthcare Materials,
Год журнала:
2024,
Номер
13(15)
Опубликована: Фев. 22, 2024
Abstract
Amyloid
beta‐protein
(AβA
β
)
is
a
main
hallmark
of
Alzheimer's
disease
(AD),
and
low
amount
Aβ
protein
accumulation
appears
to
be
potential
marker
for
AD.
Here,
an
electrochemical
DNA
biosensor
based
on
polyamide/polyaniline
carbon
nanotubes
(PA/PANI‐CNTs)
developed
with
the
aim
diagnosing
AD
early
using
simple,
low‐cost,
accessible
method
rapidly
detect
Aβ42
in
human
blood.
Electrospun
PA
nanofibers
served
as
skeleton
successive
situ
deposition
PANI
CNTs,
which
contribute
both
high
conductivity
abundant
binding
sites
aptamers.
After
aptamers
are
immobilized,
this
aptasensor
exhibits
precise
specific
detection
blood
within
only
4
min
extremely
fast
response
rate,
lower
limit,
excellent
linear
range.
These
findings
make
significant
contribution
advancing
development
serum‐based
techniques
Aβ42,
thereby
paving
way
improved
diagnostic
capabilities
field
Nature Communications,
Год журнала:
2019,
Номер
10(1)
Опубликована: Окт. 29, 2019
Abstract
The
formation
of
Aβ
amyloid
fibrils
is
a
neuropathological
hallmark
Alzheimer’s
disease
and
cerebral
angiopathy.
However,
the
structure
from
brain
tissue
poorly
understood.
Here
we
report
purification
meningeal
their
structural
analysis
with
cryo-electron
microscopy.
We
show
that
these
are
polymorphic
but
consist
similarly
structured
protofilaments.
Brain
derived
right-hand
twisted
peptide
fold
differs
sharply
previously
analyzed
were
formed
in
vitro.
These
data
underscore
importance
to
use
patient-derived
when
investigating
basis
disease.
Science,
Год журнала:
2022,
Номер
375(6577), С. 167 - 172
Опубликована: Янв. 14, 2022
Hi-res
view
of
human
Aβ42
filaments
Alzheimer’s
disease
is
characterized
by
a
loss
memory
and
other
cognitive
functions
the
filamentous
assembly
Aβ
tau
in
brain.
The
peptides
into
that
end
at
residue
42
central
event.
Yang
et
al
.
used
electron
cryo–electron
microscopy
to
determine
structures
from
brain
(see
Perspective
Willem
Fändrich).
They
identified
two
types
related
S-shaped
filaments,
each
consisting
identical
protofilaments.
These
will
inform
development
better
vitro
animal
models,
inhibitors
assembly,
imaging
agents
with
increased
specificity
sensitivity.
—SMH
Acta Neuropathologica,
Год журнала:
2015,
Номер
130(3), С. 315 - 331
Опубликована: Июль 25, 2015
The
unfolded
protein
response
(UPR)
is
a
stress
of
the
endoplasmic
reticulum
(ER)
to
disturbance
in
folding.
so-called
ER
sensors
PERK,
IRE1
and
ATF6
play
central
role
initiation
regulation
UPR.
accumulation
misfolded
aggregated
proteins
common
characteristic
neurodegenerative
diseases.
With
discovery
basic
machinery
UPR,
idea
was
born
that
UPR
or
part
its
could
be
involved
diseases
like
Alzheimer's
disease,
Parkinson's
amyotrophic
lateral
sclerosis
prion
disease.
Over
last
decade,
has
been
addressed
an
increasing
number
studies
on
neurodegeneration.
involvement
investigated
human
neuropathology
across
different
neurological
diseases,
as
well
cell
mouse
models
for
Studies
using
disease
display
discrepancies
function
during
neurodegeneration,
which
can
often
attributed
differences
methodology.
In
this
review,
we
will
address
importance
investigation
brain
material
interpretation
We
discuss
evidence
activation
methodology
study
connection
pathology
addressed.
More
recently,
recognized
target
drug
therapy
treatment
prevention
by
inhibiting
specific
mediators
Several
preclinical
have
shown
proof-of-concept
approach
targeting
particular
PERK
pathway,
neurodegeneration
yielded
paradoxical
results.
promises
held
these
observations
need
further
support
clarification
observed
between
models,
increased
insight
obtained
from
neuropathology.
Alzheimer s Research & Therapy,
Год журнала:
2020,
Номер
12(1)
Опубликована: Авг. 12, 2020
The
body
of
evidence
suggesting
a
causative,
initiating
role
beta
amyloid
(Aβ)
in
the
pathogenesis
Alzheimer's
disease
(AD)
is
substantial.
Yet,
only
few
anti-amyloid
agents
have
shown
meaningful
efficacy
clinical
trials.
We
evaluated
unifying
characteristics
with
positive
or
biomarker
effects
long-duration
trials
and
analyzed
how
pharmacological
determine
their
product
profiles.
Four
potential
for
near
term
approval
fulfill
these
criteria:
injectable
antibodies,
aducanumab,
gantenerumab,
BAN2401,
small
molecule
oral
agent,
ALZ-801.
Aducanumab
BAN2401
showed
significant
on
both
outcomes;
gantenerumab
effects,
no
reported
to
date;
ALZ-801
high-risk
population
patients
homozygous
ε4
allele
apolipoprotein
E
gene
(APOE4)
dose-dependent
preservation
hippocampal
volume.
explored
properties
agents,
namely
selectivity
Aβ
oligomers,
plasma
half-life,
brain
penetration,
time
peak
exposure,
A
crucial
characteristic
shared
by
ability
engage
neurotoxic
soluble
albeit
various
degrees.
partially
target
while
mostly
clearing
insoluble
plaques;
preferentially
targets
protofibrils
(large
oligomers)
over
blocks
formation
oligomers
without
binding
plaques.
degree
exposure
drive
magnitude
onset
efficacy,
clearance
plaques
associated
vasogenic
edema.
Only
highest
doses
aducanumab
show
modest
higher
dosing
limited
increased
risk
edema,
especially
APOE4
carriers.
These
limitations
can
be
avoided,
improved
that
selectively
inhibit
block
toxicity
most
advanced
selective
anti-oligomer
agent
ALZ-801,
an
optimized
prodrug
tramiprosate,
which
demonstrated
APOE4/4
AD
subjects.
fully
inhibits
Aβ42
at
dose,
will
phase
3
trial
early
AD.
In
addition
measures,
include
cerebrospinal
fluid,
plasma,
imaging
biomarkers
gain
further
insights
into
impact
progression.
Interface Focus,
Год журнала:
2017,
Номер
7(6), С. 20170030 - 20170030
Опубликована: Окт. 20, 2017
The
number
of
biological
therapeutic
agents
in
the
clinic
and
development
pipeline
has
increased
dramatically
over
last
decade
will
undoubtedly
continue
to
increase
coming
years.
Despite
this
fact,
there
are
considerable
challenges
development,
production
formulation
such
biologics
particularly
with
respect
their
physical
stabilities.
There
many
cases
where
self-association
form
either
amorphous
aggregates
or
highly
structured
fibrillar
species
limits
use.
Here,
we
review
numerous
factors
that
influence
stability
peptides
including
both
intrinsic
external
factors,
wherever
possible
illustrating
these
examples
interest.
effects
sequence,
concentration,
pH,
net
charge,
excipients,
chemical
degradation
modification,
surfaces
interfaces,
impurities
all
discussed.
In
addition,
parameters
as
pressure,
temperature,
agitation
lyophilization
described.
We
provide
an
overview
structures
formed,
well
our
current
knowledge
mechanisms
for
formation.
International Journal of Molecular Sciences,
Год журнала:
2016,
Номер
17(2), С. 189 - 189
Опубликована: Фев. 2, 2016
Neurodegenerative
diseases
(NDDs)
are
characterized
by
selective
dysfunction
and
loss
of
neurons
associated
with
pathologically
altered
proteins
that
deposit
in
the
human
brain
but
also
peripheral
organs.
These
their
biochemical
modifications
can
be
potentially
targeted
for
therapy
or
used
as
biomarkers.
Despite
a
plethora
demonstrated
different
neurodegeneration-related
proteins,
such
amyloid-β,
prion
protein,
tau,
α-synuclein,
TAR
DNA-binding
protein
43
(TDP-43),
fused
sarcoma
(FUS),
molecular
classification
NDDs
relies
on
detailed
morphological
evaluation
deposits,
distribution
brain,
correlation
to
clinical
symptoms
together
specific
genetic
alterations.
A
further
facet
neuropathology-based
is
fact
many
deposits
show
hierarchical
involvement
regions.
This
has
been
shown
Alzheimer
Parkinson
disease
some
forms
tauopathies
TDP-43
proteinopathies.
The
present
paper
aims
summarize
current
NDDs,
focusing
most
relevant
aspects.
Since
combination
proteinopathies
frequent,
definition
novel
clusters
patients
needs
considered
era
precision
medicine.
Optimally,
neuropathological
categorizing
should
translated
into
vivo
detectable
biomarkers
support
better
prediction
prognosis
stratification
trials.
